DNA methylation impact on Fabry disease

Risi, Teodolinda Di; Vinciguerra, Roberta; Cuomo, Mariella; Monica, Rosa Della; Riccio, Eleonora; Cocozza, Sirio; Imbriaco, Massimo; Duro, Giovanni; Pisani, Antonio; Chiariotti, Lorenzo

doi:10.1186/s13148-021-01019-3

Cited by 19 publications

(14 citation statements)

References 59 publications

(113 reference statements)

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“…Although few studies have dealt with the role of methylation in FD, for a review see Di Risi et al ( 24 ); the present study provided further evidence on the potential role of DNA methylation involvement in the clinical manifestation of FD. The GLA mutations can cause total or partial decreased activity of α-Gal A and accumulation of glycosphingolipids ( 3 , 4 ).…”

Section: Discussionsupporting

confidence: 64%

The potential consequences of bidirectional promoter methylation on GLA and HNRNPH2 expression in Fabry disease phenotypes in a family of patients carrying a GLA deletion variant

2022

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Fabry disease (FD) is a rare inherited disease characterized by a wide range of symptoms attributed to GLA mutations resulting in defective α-galactosidase A (α-Gal A) and accumulation of glycosphingolipids. The GLA locus is paired in a divergent manner with the heterogeneous nuclear ribonucleoprotein HNRNPH2 locus mapped in the RPL36A-HNRNPH2 readthrough locus. As a follow-up to our recent finding of the co-regulation of GLA and HNRNPH2 via a bidirectional promoter (BDP) in normal kidney and skin cells, the potential accumulative influence of BDP methylation and GLA mutation on the severity of FD in patients from the same family, two males and two females carrying a GLA deletion mutation, c.1033_1034delTC (p.Ser345Argfs) was addressed in the present study. The molecular analyses of the FD patients compared with the control revealed that the expression of GLA was significantly low (P<0.05), and HNRNPH2 showed a tendency of low expression (P=0.1) when BDP methylation was elevated in FD patients, compared with low BDP methylation and high GLA expression (P<0.05), and a high trend of HNRNPH2 expression in normal individuals. The accumulative effects of the mutation and BDP methylation with the severity of the disease were observed in three patients. One male FD patient, a member of the FD family diagnosed with progressive loss of kidney function, hypertension, and eventually a stroke, and the lowest level of α-Gal A enzyme activity showed the highest BDP DNA methylation level. It is concluded that the DNA methylation of GLA-HNRNPH2 BDP may serve a role in diagnosing and treating FD.

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Section: Discussionsupporting

confidence: 64%

The potential consequences of bidirectional promoter methylation on GLA and HNRNPH2 expression in Fabry disease phenotypes in a family of patients carrying a GLA deletion variant

2022

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“…Hossain et al [ 14 , 15 ] directly analyzed methylation of the GLA gene in female Fabry patients, and showed that methylation of the non-mutated allele correlated with disease severity. These studies highlighted the potential effect of methylation of GLA gene on α-gal A activity and disease phenotype in heterozygous females (for a review on the role of DNA methylation in Fabry disease, see Di Risi et al [ 16 ]). However, the role of epigenetic modifications as a downstream mediator in disease pathogenesis has not been studied.…”

Section: Introductionmentioning

confidence: 99%

Dysregulated DNA methylation in the pathogenesis of Fabry disease

Shen¹,

Balaji²,

Shigeyasu³

et al. 2022

Molecular Genetics and Metabolism Reports

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“…To investigate the DNA methylation of promoter CpG island (PCGI) associated with GBM disease progression, we established a richly computational strategy that maps the Infinium HumanMethylation450K microarray to gene PCGI methylation profiles and summarizes DNA methylation patterns at the gene level ( Zhao et al, 2021b ). First, based on the gene annotation derived from the GENCODE database and GPL13534 platform file containing the methylation probes information ( Li et al, 2020 ; Di Risi et al, 2021 ), we defined the promoter region as 2 kb located upstream of the transcription start site ( Hollstein et al, 2019 ). We extracted the relevant probes on the PCGI from the annotation file for subsequent analysis ( Carro et al, 2010 ).…”

Section: Resultsmentioning

confidence: 99%

“…Besides, we downloaded gene expression data from the Chinese Glioma Genome Atlas (CGGA, http://www.cgga.org.cn/ ) database as a supplementary dataset, which includes 282 GBM patients who possessed complete clinical information ( Zhao et al, 2021a ). The annotation file for mRNAs and promoter region was derived from the GENCODE database ( https://www.gencodegenes.org/ ) ( Di Risi et al, 2021 ). The single-cell sequencing data were obtained from GSE162631 in the GEO database, and cells derived from the tumor cores of three GBM patients in the dataset were selected ( Xie et al, 2021a ).…”

Section: Methodsmentioning

confidence: 99%

Regulatory pattern of abnormal promoter CpG island methylation in the glioblastoma multiforme classification

Wang

Zhao²,

Wang³

et al. 2022

Front. Genet.

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Glioblastoma (GBM) is characterized by extensive genetic and phenotypic heterogeneity. However, it remains unexplored primarily how CpG island methylation abnormalities in promoter mediate glioblastoma typing. First, we presented a multi-omics scale map between glioblastoma sample clusters constructed based on promoter CpG island (PCGI) methylation-driven genes, using datasets including methylation profiles, expression profiles, and single-cell sequencing data from multiple highly annotated public clinical cohorts. Second, we identified differences in the tumor microenvironment between the two glioblastoma sample clusters and resolved key signaling pathways between cell clusters at the single-cell level based on comprehensive comparative analyses to investigate the reasons for survival differences between two of these clusters. Finally, we developed a diagnostic map and a prediction model for glioblastoma, and compared theoretical differences of drug sensitivity between two glioblastoma sample clusters. In summary, this study established a classification system for dissecting promoter CpG island methylation heterogeneity in glioblastoma and provides a new perspective for the diagnosis and treatment of glioblastoma.

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DNA methylation impact on Fabry disease

Cited by 19 publications

References 59 publications

The potential consequences of bidirectional promoter methylation on GLA and HNRNPH2 expression in Fabry disease phenotypes in a family of patients carrying a GLA deletion variant

The potential consequences of bidirectional promoter methylation on GLA and HNRNPH2 expression in Fabry disease phenotypes in a family of patients carrying a GLA deletion variant

Dysregulated DNA methylation in the pathogenesis of Fabry disease

Regulatory pattern of abnormal promoter CpG island methylation in the glioblastoma multiforme classification

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